Journal article
Expression of progesterone receptor membrane component-2 within the immature rat ovary and its role in regulating mitosis and apoptosis of spontaneously immortalized granulosa cells
Biology of reproduction, Vol.91(2), pp.36-36
08/2014
Handle:
https://hdl.handle.net/2376/106889
PMID: 24990806
Abstract
Progesterone receptor membrane component 2 (Pgrmc2) mRNA was detected in the immature rat ovary. By 48 h after eCG, Pgrmc2 mRNA levels decreased by 40% and were maintained at 48 h post-hCG. Immunohistochemical studies detected PGRMC2 in oocytes and ovarian surface epithelial, interstitial, thecal, granulosa, and luteal cells. PGRMC2 was also present in spontaneously immortalized granulosa cells, localizing to the cytoplasm of interphase cells and apparently to the mitotic spindle of cells in metaphase. Interestingly, PGRMC2 levels appeared to decrease during the G1 stage of the cell cycle. Moreover, overexpression of PGRMC2 suppressed entry into the cell cycle, possibly by binding the p58 form of cyclin dependent kinase 11b. Conversely, Pgrmc2 small interfering RNA (siRNA) treatment increased the percentage of cells in G1 and M stage but did not increase the number of cells, which was likely due to an increase in apoptosis. Depleting PGRMC2 did not inhibit cellular (3)H-progesterone binding, but attenuated the ability of progesterone to suppress mitosis and apoptosis. Taken together these studies suggest that PGRMC2 affects granulosa cell mitosis by acting at two specific stages of the cell cycle. First, PGRMC2 regulates the progression from the G0 into the G1 stage of the cell cycle. Second, PGRMC2 appears to localize to the mitotic spindle, where it likely promotes the final stages of mitosis. Finally, siRNA knockdown studies indicate that PGRMC2 is required for progesterone to slow the rate of granulosa cell mitosis and apoptosis. These findings support a role for PGRMC2 in ovarian follicle development.
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Details
- Title
- Expression of progesterone receptor membrane component-2 within the immature rat ovary and its role in regulating mitosis and apoptosis of spontaneously immortalized granulosa cells
- Creators
- Daniel Griffin - Department of Obstetrics and Gynecology, University of Connecticut Health Center, Farmington, ConnecticutXiufang Liu - Department of Cell Biology, University of Connecticut Health Center, Farmington, ConnecticutCindy Pru - Center for Reproductive Biology, Department of Animal Science, Washington State University, Pullman, WashingtonJames K Pru - Center for Reproductive Biology, Department of Animal Science, Washington State University, Pullman, WashingtonJohn J Peluso - Department of Cell Biology, University of Connecticut Health Center, Farmington, Connecticut Department of Obstetrics and Gynecology, University of Connecticut Health Center, Farmington, Connecticut peluso@nso2.uchc.edu
- Publication Details
- Biology of reproduction, Vol.91(2), pp.36-36
- Academic Unit
- Animal Sciences, Department of
- Publisher
- United States
- Grant note
- R01 HD052740 / NICHD NIH HHS R21 HD066297 / NICHD NIH HHS R21 RR030264 / NCRR NIH HHS
- Identifiers
- 99900546533501842
- Language
- English
- Resource Type
- Journal article